1,2-Amino oxygenation of alkenes with hydrogen evolution reaction

1,2-Amino oxygenation of alkenes has emerged as one of the most straightforward synthetic methods to produce β-amino alcohols, which are important organic building blocks. Thus, a practical synthetic strategy for 1,2-amino oxygenation is highly desirable. Here, we reported an electro-oxidative intermolecular 1,2-amino oxygenation of alkenes with hydrogen evolution, removing the requirement of extra-oxidant. Using commercial oxygen and nitrogen sources as starting materials, this method provides a cheap, scalable, and efficient route to a set of valuable β-amino alcohol derivatives. Moreover, the merit of this protocol has been exhibited by its broad substrate scope and good application in continuous-flow reactors. Furthermore, this method can be extended to other amino-functionalization of alkenes, thereby showing the potential to inspire advances in applications of electro-induced N-centered radicals (NCRs).

Although numerous attractive methods have been developed for this ideal synthesis, several challenges still remain in the 1,2-amino oxygenation approach (Fig. 1b) 6 . One internal challenge is the precise control of regio-and chemoselectivity in this transformation. Since the reacting oxygen and nitrogen nucleophiles generally showed similar reactivity, other potential reactions, including diamination, 1,2-oxyamination, and dioxygenation, might adversely affect the desired 1,2-amino oxygenation. Another challenge in the application is the development of mild methods with good compatibility for both oxygen and nitrogen sources, especially for O-H and N-H compounds that represent a direct and atom-economical route. Thus, developing an efficient, cheap, and easy-to-handle method to Based on our previous works on electro-induced NCR chemistry 37-39 , we conceived a feasible electro-oxidative 1,2-amino oxygenation of alkenes to address these challenges (Fig. 1c). As the initiation of this hypothesis, an anti-Markovnikov addition between NCRs and alkenes can provide high regioselectivity for such organic transformation. Moreover, the hydrogen evolution in the cathode can increase the concentration of alkoxy anions ( -OR), which may further promote the formation of C-O bonds. Meanwhile, the direct utilization of O-H and N-H compounds may ensure the wide applicability of this synthetic method. Therefore, we report here an efficient, transition-metal-catalyst-and oxidant-free alkenes 1,2amino oxygenation via an electro-induced NCRs pathway, providing a practical route toward synthesizing β-amino alcohol derivatives.

Condition optimization for electro-oxidative 1,2-amino oxygenation
Usually, solvents affect the lifetime and reactivity of NCRs. Therefore, various solvents involving O-H functionalities were initially examined with N-methyl-p-toluenesulfonamide 1a and styrene 2aa as the model substrates. Unfortunately, the desired 1,2-amino oxygenation products were not detected in AcOH, EtOH, 2,2,2-trifluoroethanol (TFE), and hexafluoroisopropanol (HFIP) (see Supplementary Table 1). Though the 1,2-amino oxygenation was successfully achieved in MeOH, those tested reactions were limited in their moderate yields (see details in Supplementary Table 2). Combined with our previous works, the mixed solvents were attempted, including dichloromethane (DCM)/TFE, MeCN/ TFE, and DCM/HFIP. When the mixture of DCM (4 mL) and TFE 3 (2 mL) was used, the 1,2-amino oxygenation was successfully accomplished to form target product 4aa in 76% isolated yield by using 2 equivalents 1,8diazabicyclo [5.4.0]undec-7-ene (DBU) as the base (Table 1, entry 1). DBU is essential for the high yield, as the low conversion of 1aa and no target product detected in its absence (entry 2), while lower yields were obtained with the use of K 3 PO 4 or Cs 2 CO 3 instead of DBU (entries 3 and 4). The separated yield of 4aa slightly reduced when the electron current was decreased to 2 mA or increased to 10 mA, even with the same electron quantity (entries 5 and 6). The utilization of carbon rod or Ni plate as cathode could also furnish the product 4aa, but in lower yields (entries 7 and 8). This electro-chemical conversion was compatible with air in which the products were formed in 60% yield (entry 9). The control experiment showed that the current is necessary for this transformation (entry 10).

Scope of substrates
With the optimized protocol for alkene 1,2-amino oxygenation, we examined the scope of alkenes using N-methyl-p-toluenesulfonamide   1aa in the mixture of DCM and TFE (Fig. 2a). Various monofunctionalized styrenes with ortho-, metaor para-substituents were suitable radical acceptors to afford the corresponding products in moderate to good yields (4aa-4am). Notably, though alkenes with electron-withdrawing groups transformed to the target products smoothly (4an and 4ao), this 1,2-amino oxygenation was completed in low yields using alkenes with strong electron-donating groups (4ap and 4aq) or naphthalene (4ar). In addition, alkene with a sensitive functional group, for example, benzyl chloride, was well tolerated in this condition (4as). Moreover, alkenyl ether derivatives were also compatible with this electro-oxidative 1,2-amino oxygenation. Various alkenyl ethers were smoothly transformed to target products in moderate yields (4at-4ba). In addition, unactivated 1,1-disubstituted alkene 2bb successfully realized amino oxygenation to afford products 4bb.
Subsequently, further exploration of sulfonamides was carried out under electro-oxidative conditions (Fig. 2b). A series of functionalized benzenesulfonamides with electron-donating or electronwithdrawing groups were satisfactory amination reagents (5a-5j). Moreover, sulfonamides with (hetero)cyclic motifs were also suitable for producing products in moderate yields (5k-5m). Furthermore, other N-alkyl substituted sulfonamides well performed in this 1,2amino oxygenation (5n-5r). With the respect to limitation, secondary alkylamines and primary amides failed toward the target products under the optimized conditions. When the activated methylene was present on the nitrogen atom, the amino oxygenation was also achieved in low yields (5s, 5t). More efforts to address these limitations are currently going on.

Strategic expansions and synthetic applications
Next, a series of experiments were performed to demonstrate the expansion of this strategy (Fig. 3A). Additional scope of alkenes with HOAc illustrated that this method could be well expanded to other acids with good functional group compatibility ( Fig. 3A-a, 6a-6j). In addition, this electro-induced alkenes di-functionalizations were successfully achieved with other nucleophiles, including acids, alcohols, and even pyrazoles ( Fig. 3A-b, 6k-6s).
To show the potential in further application, this synthetic method was also demonstrated in a continuous-flow reactor (Fig. 3Bc). At the flow rate of 0.8 mL min −1 , the desired 1,2-amino oxygenation was completed smoothly to produce 1.88 g products in 81% isolated yield. In addition, 4ba and 6a were also well performed in continuousflow conditions toward a gram-scale synthesis of β-amino alcohol derivatives. Furthermore, this transformation was applied in the synthesis of 8, which could further furnish a natural product, halostachine (Fig. 3B-d) 40 .

Mechanistic studies
Then, several experiments were carried out to explore the mechanism of this electro-chemical 1,2-amino oxygenation (Fig. 4A). As shown in Fig. 4A-a, the NMR experiments supported a proton transfer progress between 1a and DBU before electro-induced progress. When sulfonamides 10 was utilized for this transformation under standard conditions (Fig. 4A-b), both desired 1,2-amino oxygenation product 10a and a intramolecular cyclization product 10b via Hofmann-Löffler-Freytag reaction were obtained. These results supported the involvement of NCRs progress in the reaction system 37,41 . In addition, the radical clock experiment was carried out with the use of alkene 11 (Fig. 4A-c). The formation of the corresponding ring-opening adduct 11a further supported the radical addition of in-situ formed NCRs to alkenes. Afterward, a series of CV studies were performed to explore the anodic reaction ( Fig. 4A-d).
Although the oxidative peak of 1a was not observed in the range of 0-2.5 V, the catalytic current of DBU obviously increased with the addition of 1a. These results revealed that DBU was electroactive, supporting a fast electron-transfer progress between oxidized DBU and 1a. While styrene 2aa showed an electro-redox activity, styrenes with electron-donating groups led to low yields ( Supplementary  Fig. 6). Therefore, the direct oxidation of alkenes may not be the initial step of this electro-oxidative transformation.
Based on the above results and previous studies 37,39 , a plausible mechanism was proposed for this electro-oxidative 1,2-amino oxygenation (Fig. 4B). Firstly, a proton transfer between sulfonamide 1a and DBU happened to generate N-centered anion I, which could be oxidized toward NCR II in the anode. Another mechanism could not be ruled out that a mixture of 1a and DBU was directly oxidized in the anode to afford NCR II. Subsequently, such NCR II was added to the alkene 2a to form a C-centered radical III, which could further be oxidized for the formation of C-centered cation IV. Then intermediate IV was attacked by trifluoroethanol 3 with the release of a proton. In the cathode, two protons were reducted to evolute hydrogen.
In summary, we have developed an electro-oxidative 1,2-amino oxygenation of alkenes using readily available sulfonamides and alcohols as nitrogen and oxygen sources with H 2 evolution. This method offers a convenient and powerful synthetic approach toward β-amino alcohols in one step without extra-oxidants. Moreover, the wide scope, good performance in continuous-flow electro-reactor, and the efficient synthesis of natural products illustrate the potential applicability of this method in the industry. Furthermore, this method can be extended to other alkene amino-functionalizations, thereby having the potential to inspire advances in other transformations via electro-induced NCRs.

Methods
In an oven-dried undivided three-necked bottle (10 mL) equipped with a stir bar, sulfonamide substrate 1a (0.3 mmol) and n Bu 4 NBF 4 (0.3 mmol) were combined and added. The undivided cell was equipped with graphite rod anode (ф 6 mm), platinum plate cathode (1.5 cm × 1.5 cm × 0.3 mm) and was then charged with nitrogen. Under the atmosphere of nitrogen, DBU (0.6 mmol), and alkenes 2 (0.9 mmol) were added, then DCM (4.0 mL) and TFE (2.0 mL) were injected respectively into the tubes via syringes. The mixture was electrolyzed using constant current conditions (4.0 mA) for 5 h at room temperature under magnetic stirring. When TLC analysis indicated that the electrolysis was complete (witnessed by the disappearance of the 1a), the solvent was removed under reduced pressure. The residue was purified by column chromatography on silica gel using a mixture of PE/EA (v:v = 25:1) as eluent to afford the desired pure product. Article https://doi.org/10.1038/s41467-022-32084-8